Global Initiative for Asthma (GINA) What’s new in GINA 2016?

Global Initiative for Asthma (GINA) What’s new in GINA 2016? ... dose ICS) Moderate asthma: well-controlled with Step 3 (low-dose ICS/LABA)...

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Global Initiative for Asthma (GINA) What’s new in GINA 2016?

GINA Global Strategy for Asthma Management and Prevention © Global Initiative for Asthma

GINA: A Brief History     

Established in 1993 Collaboration between NHLBI and WHO Multiple updates since 1993 Meetings to discuss changes twice yearly Latest revision 2016

© Global Initiative for Asthma

GINA: Objectives      

Increase awareness of asthma and its public health consequences Promote identification of reasons for increased prevalence of asthma Promote study of asthma Reduce asthma morbidity and mortality Improve management of asthma Improve availability and accessibility of effective asthma therapy

© Global Initiative for Asthma

GINA Global Strategy for Asthma Management and Prevention Not a guideline, but a practical approach to managing asthma in clinical practice  A global strategy, relevant to both low and high resource countries  Evidence-based and clinically-oriented  Provides clinical tools and measurable outcomes 

GINA 2016

© Global Initiative for Asthma

Assessing asthma severity 

How?  Asthma severity is assessed retrospectively from the level of treatment required to control symptoms and exacerbations



When?  Assess asthma severity after patient has been on controller treatment for several months  Severity is not static – it may change over months or years, or as different treatments become available



Categories of asthma severity  Mild asthma: well-controlled with Steps 1 or 2 (as-needed SABA or low dose ICS)  Moderate asthma: well-controlled with Step 3 (low-dose ICS/LABA)  Severe asthma: requires Step 4/5 (moderate or high dose ICS/LABA ± add-on), or remains uncontrolled despite this treatment

GINA 2016

© Global Initiative for Asthma

Goals of asthma management 

The long-term goals of asthma management are 1. 2. 3.



Symptom control: to achieve good control of symptoms and maintain normal activity levels Risk reduction: to minimize future risk of exacerbations, fixed airflow limitation and medication side-effects Note: no mention of lung function here; use for diagnosis

Achieving these goals requires a partnership between patient and their health care providers  Ask the patient about their own goals regarding their asthma  Good communication strategies are essential  Consider the health care system, medication availability, cultural and personal preferences and health literacy

GINA 2016

© Global Initiative for Asthma

Treating to control symptoms and minimize risk  

Establish a patient-doctor partnership Manage asthma in a continuous cycle:  Assess  Adjust treatment (pharmacological and non-pharmacological)  Review the response



Teach and reinforce essential skills  Inhaler skills  Adherence  Guided self-management education • Written asthma action plan • Self-monitoring • Regular medical review

GINA 2016

© Global Initiative for Asthma

The control-based asthma management cycle Diagnosis Symptom control & risk factors (including lung function) Inhaler technique & adherence Patient preference Symptoms Exacerbations Side-effects Patient satisfaction Lung function

Asthma medications Non-pharmacological strategies Treat modifiable risk factors

GINA 2016, Box 3-2

© Global Initiative for Asthma

Stepwise management - pharmacotherapy

UPDATED!

Diagnosis Symptom control & risk factors (including lung function) Inhaler technique & adherence Patient preference Symptoms Exacerbations Side-effects

Asthma medications

Patient satisfaction

Non-pharmacological strategies

Lung function

Treat modifiable risk factors

STEP 5 STEP 4 STEP 3 PREFERRED CONTROLLER CHOICE

STEP 1

Low dose ICS Other controller options RELIEVER

Consider low dose ICS

Refer for add-on treatment

STEP 2

Leukotriene receptor antagonists (LTRA) Low dose theophylline*

As-needed short-acting beta2-agonist (SABA)

GINA 2016, Box 3-5 (2/8) (upper part)

Low dose ICS/LABA**

Med/high ICS/LABA

e.g. tiotropium,* omalizumab, mepolizumab*

Med/high dose ICS Add tiotropium* Add low Low dose ICS+LTRA High dose ICS dose OCS + LTRA (or + theoph*) (or + theoph*)

As-needed SABA or low dose ICS/formoterol#

*Not for children <12 years **For children 6-11 years, the preferred Step 3 treatment is medium dose ICS #For patients prescribed BDP/formoterol or BUD/ formoterol maintenance and reliever therapy

 Tiotropium by mist inhaler is an add-on treatment for patients ≥12 years with a history of exacerbations

© Global Initiative for Asthma

Stepwise treatment for adults and adolescents 

Step 3  Low-dose fluticasone furoate/vilanterol an option for Step 3



Step 4  Tiotropium now an add-on option for adolescents (age ≥12 years) as well as adults, with a history of exacerbations



Step 5: refer for expert investigation and add-on treatment, such as:  Add-on tiotropium by mist inhaler for patients age ≥12 years with a history of exacerbations  Add-on omalizumab (anti-IgE) for severe allergic asthma  Add-on mepolizumab (anti-IL5) for severe eosinophilic asthma (≥12 years)  Sputum-guided treatment, if available



Low, medium and high ICS doses  Fluticasone furoate: 100mcg (low dose); 200mcg (high dose)



Stepping down ICS when asthma well-controlled now Evidence A  (Hagan et al, Allergy 2014)

What’s new in GINA 2016

© Global Initiative for Asthma

Step 1 – as-needed inhaled short-acting beta2-agonist (SABA) STEP 5 STEP 4 PREFERRED CONTROLLER CHOICE

STEP 1

STEP 2

Low dose ICS Other controller options

RELIEVER

Consider low dose ICS

Leukotriene receptor antagonists (LTRA) Low dose theophylline*

As-needed short-acting beta2-agonist (SABA)

Refer for add-on treatment

STEP 3

Low dose ICS/LABA** Med/high dose ICS Low dose ICS+LTRA (or + theoph*)

Med/high ICS/LABA

Add tiotropium* High dose ICS + LTRA (or + theoph*)

e.g. tiotropium,* omalizumab, mepolizumab*

Add low dose OCS

As-needed SABA or low dose ICS/formoterol#

*Not for children <12 years **For children 6-11 years, the preferred Step 3 treatment is medium dose ICS #For patients prescribed BDP/formoterol or BUD/ formoterol maintenance and reliever therapy  Tiotropium by mist inhaler is an add-on treatment for patients ≥12 years with a history of exacerbations

GINA 2016, Box 3-5, Step 1 (4/8)

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Step 1 – as-needed reliever inhaler 

Preferred option: as-needed inhaled short-acting beta2-agonist (SABA)  SABAs are highly effective for relief of asthma symptoms  However …. there is insufficient evidence about the safety of treating asthma with SABA alone  This option should be reserved for patients with infrequent symptoms (less than twice a month) of short duration, and with no risk factors for exacerbations



Other options  Consider adding regular low dose inhaled corticosteroid (ICS) for patients at risk of exacerbations

GINA 2016

© Global Initiative for Asthma

Step 2 – low-dose controller + as-needed inhaled SABA

STEP 5 STEP 4 PREFERRED CONTROLLER CHOICE

STEP 1

STEP 2

Low dose ICS Other controller options

RELIEVER

Consider low dose ICS

Leukotriene receptor antagonists (LTRA) Low dose theophylline*

As-needed short-acting beta2-agonist (SABA)

Refer for add-on treatment

STEP 3

Low dose ICS/LABA**

Med/high ICS/LABA

Med/high dose ICS Add tiotropium* Low dose ICS+LTRA High dose ICS (or + theoph*) + LTRA (or + theoph*)

e.g. tiotropium,* omalizumab, mepolizumab*

Add low dose OCS

As-needed SABA or low dose ICS/formoterol#

*Not for children <12 years **For children 6-11 years, the preferred Step 3 treatment is medium dose ICS #For patients prescribed BDP/formoterol or BUD/ formoterol maintenance and reliever therapy  Tiotropium by mist inhaler is an add-on treatment for patients ≥12 years with a history of exacerbations

GINA 2016, Box 3-5, Step 2 (5/8)

© Global Initiative for Asthma

Step 2 – Low dose controller + as-needed SABA 

Preferred option: regular low dose ICS with as-needed inhaled SABA  Low dose ICS reduces symptoms and reduces risk of exacerbations and asthma-related hospitalization and death



Other options 

Leukotriene receptor antagonists (LTRA) with as-needed SABA • Less effective than low dose ICS • May be used for some patients with both asthma and allergic rhinitis, or if patient will not use ICS

 Combination low dose ICS/long-acting beta2-agonist (LABA) with as-needed SABA • Reduces symptoms and increases lung function compared with ICS • More expensive, and does not further reduce exacerbations

 Intermittent ICS with as-needed SABA for purely seasonal allergic asthma with no interval symptoms • Start ICS immediately symptoms commence, and continue for 4 weeks after pollen season ends

GINA 2016

© Global Initiative for Asthma

Step 3 – one or two controllers + as-needed inhaled reliever

STEP 5 STEP 4 PREFERRED CONTROLLER CHOICE

STEP 1

STEP 2

Low dose ICS Other controller options

RELIEVER

Consider low dose ICS

Leukotriene receptor antagonists (LTRA) Low dose theophylline*

As-needed short-acting beta2-agonist (SABA)

Refer for add-on treatment

STEP 3

Low dose ICS/LABA**

Med/high ICS/LABA

Med/high dose ICS Add tiotropium* Low dose ICS+LTRA High dose ICS + LTRA (or + theoph*) (or + theoph*)

e.g. tiotropium,* omalizumab, mepolizumab*

Add low dose OCS

As-needed SABA or low dose ICS/formoterol#

*Not for children <12 years **For children 6-11 years, the preferred Step 3 treatment is medium dose ICS #For patients prescribed BDP/formoterol or BUD/ formoterol maintenance and reliever therapy  Tiotropium by mist inhaler is an add-on treatment for patients ≥12 years with a history of exacerbations

GINA 2016, Box 3-5, Step 3 (6/8)

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Step 3 – one or two controllers + as-needed inhaled reliever 

Before considering step-up  Check inhaler technique and adherence, confirm diagnosis



Adults/adolescents: preferred options are either combination low dose ICS/LABA maintenance with as-needed SABA, OR combination low dose ICS/formoterol maintenance and reliever regimen*  Adding LABA reduces symptoms and exacerbations and increases FEV1, while allowing lower dose of ICS  In at-risk patients, maintenance and reliever regimen significantly reduces exacerbations with similar level of symptom control and lower ICS doses compared with other regimens

Children 6-11 years: preferred option is medium dose ICS with as-needed SABA  Other options 

 Adults/adolescents: Increase ICS dose or add LTRA or theophylline (less effective than ICS/LABA)  Children 6-11 years – add LABA (similar effect as increasing ICS) *Approved only for low dose beclometasone/formoterol and low dose budesonide/formoterol GINA 2016

© Global Initiative for Asthma

Step 4 – two or more controllers + as-needed inhaled reliever

STEP 5 STEP 4 PREFERRED CONTROLLER CHOICE

STEP 1

STEP 2

Low dose ICS Other controller options

RELIEVER

Consider low dose ICS

Leukotriene receptor antagonists (LTRA) Low dose theophylline*

As-needed short-acting beta2-agonist (SABA)

Refer for add-on treatment

STEP 3

Low dose ICS/LABA**

Med/high ICS/LABA

Med/high dose ICS Add tiotropium* Low dose ICS+LTRA High dose ICS + LTRA (or + theoph*) (or + theoph*)

e.g. tiotropium,* omalizumab, mepolizumab*

Add low dose OCS

As-needed SABA or low dose ICS/formoterol#

*Not for children <12 years **For children 6-11 years, the preferred Step 3 treatment is medium dose ICS #For patients prescribed BDP/formoterol or BUD/ formoterol maintenance and reliever therapy  Tiotropium by mist inhaler is an add-on treatment for patients ≥12 years with a history of exacerbations

GINA 2016, Box 3-5, Step 4 (7/8)

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Step 4 – two or more controllers + as-needed inhaled reliever 

Before considering step-up  Check inhaler technique and adherence



 

Adults or adolescents: preferred option is combination low dose ICS/formoterol as maintenance and reliever regimen*, OR combination medium dose ICS/LABA with as-needed SABA Children 6–11 years: preferred option is to refer for expert advice Other options (adults or adolescents)  Tiotropium by mist inhaler may be used as add-on therapy for patients aged ≥12 years with a history of exacerbations  Trial of high dose combination ICS/LABA, but little extra benefit and increased risk of side-effects  Increase dosing frequency (for budesonide-containing inhalers)  Add-on LTRA or low dose theophylline

*Approved only for low dose beclometasone/formoterol and low dose budesonide/formoterol GINA 2016

© Global Initiative for Asthma

Step 5 – higher level care and/or add-on treatment

UPDATED!

STEP 5 STEP 4 PREFERRED CONTROLLER CHOICE

STEP 1

STEP 2

Low dose ICS Other controller options

RELIEVER

Consider low dose ICS

Leukotriene receptor antagonists (LTRA) Low dose theophylline*

As-needed short-acting beta2-agonist (SABA)

Refer for add-on treatment

STEP 3

Low dose ICS/LABA**

Med/high ICS/LABA

Med/high dose ICS Add tiotropium* Low dose ICS+LTRA High dose ICS + LTRA (or + theoph*) (or + theoph*)

e.g. tiotropium,* omalizumab, mepolizumab*

Add low dose OCS

As-needed SABA or low dose ICS/formoterol#

*Not for children <12 years **For children 6-11 years, the preferred Step 3 treatment is medium dose ICS #For patients prescribed BDP/formoterol or BUD/ formoterol maintenance and reliever therapy  Tiotropium by mist inhaler is an add-on treatment for patients ≥12 years with a history of exacerbations

GINA 2016, Box 3-5, Step 5 (8/8)

© Global Initiative for Asthma

Step 5 – higher level care and/or add-on treatment 

UPDATED!

Preferred option is referral for specialist investigation and consideration of add-on treatment  If symptoms uncontrolled or exacerbations persist despite Step 4 treatment, check inhaler technique and adherence before referring  Add-on tiotropium for patients ≥12 years with history of exacerbations  Add-on omalizumab (anti-IgE) for patients with severe allergic asthma  Add-on mepolizumab (anti-IL5) for severe eosinophilic asthma (≥12 yrs)



Other add-on treatment options at Step 5 include:  Sputum-guided treatment: available in specialized centers; reduces exacerbations and/or corticosteroid dose  Add-on low dose oral corticosteroids (≤7.5mg/day prednisone equivalent): this may benefit some patients, but has significant systemic side-effects. Assess and monitor for osteoporosis  See ERS/ATS Severe Asthma Guidelines (Chung et al, ERJ 2014) for more detail

GINA 2016

© Global Initiative for Asthma

Low, medium and high dose inhaled corticosteroids Adults and adolescents (≥12 years)

UPDATED!

Total daily dose (mcg)

Inhaled corticosteroid Low

Medium

High

Beclometasone dipropionate (CFC)

200–500

>500–1000

>1000

Beclometasone dipropionate (HFA)

100–200

>200–400

>400

Budesonide (DPI)

200–400

>400–800

>800

Ciclesonide (HFA)

80–160

>160–320

>320

100

n.a.

200

Fluticasone propionate (DPI or HFA)

100–250

>250–500

>500

Mometasone furoate

110–220

>220–440

>440

400–1000

>1000–2000

>2000

Fluticasone furoate (DPI)

Triamcinolone acetonide

 This is not a table of equivalence, but of estimated clinical comparability  Most of the clinical benefit from ICS is seen at low doses  High doses are arbitrary, but for most ICS are those that, with prolonged use, are associated with increased risk of systemic side-effects GINA 2016, Box 3-6 (1/2)

© Global Initiative for Asthma

Low, medium and high dose inhaled corticosteroids Children 6–11 years Inhaled corticosteroid

Total daily dose (mcg) Low

Medium

High

Beclometasone dipropionate (CFC)

100–200

>200–400

>400

Beclometasone dipropionate (HFA)

50–100

>100–200

>200

Budesonide (DPI)

100–200

>200–400

>400

Budesonide (nebules)

250–500

>500–1000

>1000

Ciclesonide (HFA)

80

>80–160

>160

Fluticasone furoate (DPI)

n.a.

n.a.

n.a.

Fluticasone propionate (DPI)

100–200

>200–400

>400

Fluticasone propionate (HFA)

100–200

>200–500

>500

110

≥220–<440

≥440

400–800

>800–1200

>1200

Mometasone furoate Triamcinolone acetonide

 This is not a table of equivalence, but of estimated clinical comparability  Most of the clinical benefit from ICS is seen at low doses  High doses are arbitrary, but for most ICS are those that, with prolonged use, are associated with increased risk of systemic side-effects GINA 2016, Box 3-6 (2/2)

© Global Initiative for Asthma

Reviewing response and adjusting treatment 

How often should asthma be reviewed?  1-3 months after treatment started, then every 3-12 months  During pregnancy, every 4-6 weeks  After an exacerbation, within 1 week



Stepping up asthma treatment  Sustained step-up, for at least 2-3 months if asthma poorly controlled • Important: first check for common causes (symptoms not due to asthma, incorrect inhaler technique, poor adherence)

 Short-term step-up, for 1-2 weeks, e.g. with viral infection or allergen • May be initiated by patient with written asthma action plan

 Day-to-day adjustment • For patients prescribed low-dose ICS/formoterol maintenance and reliever regimen* 

Stepping down asthma treatment  Consider step-down after good control maintained for 3 months  Find each patient’s minimum effective dose, that controls both symptoms and exacerbations

*Approved only for low dose beclometasone/formoterol and low dose budesonide/formoterol GINA 2016

© Global Initiative for Asthma

General principles for stepping down controller treatment 

Aim  To find the lowest dose that controls symptoms and exacerbations, and minimizes the risk of side-effects



When to consider stepping down  When symptoms have been well controlled and lung function stable for ≥3 months  No respiratory infection, patient not travelling, not pregnant



Prepare for step-down  Record the level of symptom control and consider risk factors  Make sure the patient has a written asthma action plan  Book a follow-up visit in 1-3 months



Step down through available formulations  Stepping down ICS doses by 25–50% at 3 month intervals is feasible and safe for most patients (Hagan et al, Allergy 2014)  See GINA 2016 report Box 3-7 for specific step-down options



Stopping ICS is not recommended in adults with asthma because of risk of exacerbations (Rank et al, JACI 2013)

GINA 2016, Box 3-7

© Global Initiative for Asthma

Treating modifiable risk factors 

Provide skills and support for guided asthma self-management  This comprises self-monitoring of symptoms and/or PEF, a written asthma action plan and regular medical review



Prescribe medications or regimen that minimize exacerbations  ICS-containing controller medications reduce risk of exacerbations  For patients with ≥1 exacerbations in previous year, consider low-dose ICS/formoterol maintenance and reliever regimen*



Encourage avoidance of tobacco smoke (active or ETS)  Provide smoking cessation advice and resources at every visit



For patients with severe asthma  Refer to a specialist center, if available, for consideration of add-on medications and/or sputum-guided treatment



For patients with confirmed food allergy:  Appropriate food avoidance  Ensure availability of injectable epinephrine for anaphylaxis

*Approved only for low dose beclometasone/formoterol and low dose budesonide/formoterol GINA 2016, Box 3-8

© Global Initiative for Asthma

Non-pharmacological interventions 

Avoidance of tobacco smoke exposure  Provide advice and resources at every visit; advise against exposure of children to environmental tobacco smoke (house, car)



Physical activity  Encouraged because of its general health benefits. Provide advice about exercise-induced bronchoconstriction



Occupational asthma  Ask patients with adult-onset asthma about work history. Remove sensitizers as soon as possible. Refer for expert advice, if available



Avoid medications that may worsen asthma  Always ask about asthma before prescribing NSAIDs or beta-blockers



Remediation of dampness or mold in homes

UPDATED!

 Reduces asthma symptoms and medication use in adults 

(Allergen avoidance)  (Not recommended as a general strategy for asthma)

This slide shows examples of interventions with high quality evidence GINA 2016, Box 3-9

© Global Initiative for Asthma

Indications for considering referral, where available 

Difficulty confirming the diagnosis of asthma  Symptoms suggesting chronic infection, cardiac disease, etc  Diagnosis unclear even after a trial of treatment  Features of both asthma and COPD, if in doubt about treatment



Suspected occupational asthma  Refer for confirmatory testing, identification of sensitizing agent, advice about eliminating exposure, pharmacological treatment



Persistent uncontrolled asthma or frequent exacerbations  Uncontrolled symptoms or ongoing exacerbations or low FEV1 despite correct inhaler technique and good adherence with Step 4  Frequent asthma-related health care visits



Risk factors for asthma-related death  Near-fatal exacerbation in past  Anaphylaxis or confirmed food allergy with asthma

GINA 2016, Box 3-10 (1/2)

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Indications for considering referral, where available 

Significant side-effects (or risk of side-effects)  Significant systemic side-effects  Need for oral corticosteroids long-term or as frequent courses



Symptoms suggesting complications or sub-types of asthma  Nasal polyposis and reactions to NSAIDS (may be aspirin exacerbated respiratory disease)  Chronic sputum production, fleeting shadows on CXR (may be allergic bronchopulmonary aspergillosis)



Additional reasons for referral in children 6-11 years    

Doubts about diagnosis, e.g. symptoms since birth Symptoms or exacerbations remain uncontrolled Suspected side-effects of treatment, e.g. growth delay Asthma with confirmed food allergy

GINA 2016, Box 3-10 (2/2)

© Global Initiative for Asthma

Management of asthma in low-resource settings 

Where?  Low-resource settings may be found not only in low and middle income countries (LMIC), but also in affluent nations



Diagnosis in low-resource settings  Up to 50% asthma undiagnosed, up to 34% over-diagnosed (José 2014)  Ask about symptoms suggestive of chronic respiratory infections e.g. TB  Peak flow meters recommended by WHO as essential tools for Package of Essential Non-communicable Diseases Interventions (WHO-PEN)



Management of asthma in low-resource settings  GINA strategy for stepwise treatment includes options for low-resource settings  Prioritize the most cost-effective approach; include ICS and SABA  Build capacity of primary health care teams, including nurses and pharmacist  WHO-PEN recommends inclusion of peak flow meters as essential tools, and oximeters if resources permit

What’s new in GINA 2016

© Global Initiative for Asthma

Primary prevention of asthma (GINA Chapter 7) 

Maternal diet in pregnancy  No firm evidence that ingestion of any specific foods in pregnancy increases risk for asthma  Instead, maternal intake of foods commonly considered allergenic (peanut, milk) is associated with a decrease in allergy and asthma in offspring (Bunyavanich et al, JACI 2014; Maslova et al, JACI 2012, 2013)

 Therefore, no dietary changes are recommended during pregnancy for prevention of allergies or asthma 

Maternal obesity in pregnancy  Maternal obesity and maternal weight gain in pregnancy are associated with an increased risk for asthma in children (Forno et al, Pediatrics 2014)  However, no recommendations can be made at present, as unguided weight loss in pregnancy should not be encouraged



Dampness and mold  For children at risk of asthma, dampness, visible mold and mold odor in the home are associated with increased risk of developing asthma (Quansah et al, PLoS ONE 2012)

What’s new in GINA 2016

© Global Initiative for Asthma

Other changes in GINA 2016 

Non-pharmacological strategies for people with asthma  Remediation of dampness or mold in homes reduces asthma symptoms and medication use in adults (Evidence A) (Sauni et al, Cochrane 2015)



Other therapies  In randomized controlled trials, Vitamin D supplementation has not been associated with improvement in asthma symptom control or reduction in exacerbations • This statement was included in the GINA report because there had been wide expectation from cross-sectional studies that Vitamin D supplementation would be beneficial for asthma control

 Sections on allergen immunotherapy, vaccinations and bronchial thermoplasty have been included in the main report (previously only in Appendix) 

Methodology  More details provided about GINA methodology, including the number of articles identified at each step

What’s new in GINA 2016

© Global Initiative for Asthma

Management of severe asthma 

Optimize dose of ICS/LABA  Complete resistance to ICS is rare  Consider therapeutic trial of higher dose



Consider low dose maintenance oral corticosteroids  Monitor for and manage side-effects, including osteoporosis



Add-on treatments without phenotyping  Tiotropium - reduces exacerbations (history of exacerbations, age ≥12 years)  Theophylline, LTRA – limited benefit



Phenotype-guided treatment    



Severe allergic asthma: add-on omalizumab (anti-IgE) UPDATED! Severe eosinophilic asthma: add-on mepolizumab (anti-IL5) Sputum-guided treatment to reduce exacerbations and/or steroid dose Aspirin-exacerbated respiratory disease: consider add-on LTRA

Non-pharmacological interventions  Consider bronchial thermoplasty for selected patients  Comprehensive adherence-promoting program



For detailed guidelines, see Chung et al, ERJ 2014

GINA 2016, Box 3-14 (2/2)

© Global Initiative for Asthma

EPR-3 (2007) Differs from GINA (2016)       

Longer and more detailed Extensive discussion of underlying pathophysiology and disease mechanisms Severity assessed before starting therapy Greater emphasis on lung function testing (spirometry) and attaining normal or near normal lung function Separates assessment of asthma severity from asthma control Severity based on 6 steps (5 for GINA); control is well controlled, not well controlled, very poorly controlled Medications not updated – tiotropium, biologics, new longer acting beta agonists, etc.

© Global Initiative for Asthma

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